Publication: Importance of novel sequence alterations in the FHIT gene on formation of breast cancer
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Date
2007-03-07
Authors
Bilgel, Nazan
Tolunay, Şahsine
Taşdelen, İsmet
Tunca, Berrin
Egeli, U.
Çeçener, Gülşah
Authors
Journal Title
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Volume Title
Publisher
Sage Publications
Abstract
Aims and background: The character, role and impact of FHIT gene alterations, for which recent studies have shown that the gene has a role in the early stage of carcinogenesis in breast cancer, are still unclear. Thus, the current study evaluated FHIT gene mutations from breast tissue of women with malignant and benign breast disease and to elucidate the frequency and type of mutations in this gene. Patients and methods: Mutations in exons 5-9 of the FHIT gene were screened using the intronic primer pairs in 83 breast (67 malignant and 16 benign) tissue samples by single-strand conformational polymorphism and sequencing analysis. Results: FHIT mutations were detected in 13 of the 67 malignant cases (19.4%) and 2 of the 16 benign cases (12.5%). Four different sequence variants were determined: two novel frame shift mutations (codon 90 insA, codon 146 deIT), one intronic novel mutation (IVS8 -17 insA), and one previously identified silent transition type alteration (codon 88 C to T). In addition, determination of this silent alteration caused formation of new exonic splicing enhancer (ESE) motifs on mutated sequences by using the ESEfinder program. Conclusions: Our data contribute significantly to that currently known about the presence of FHIT gene mutations on the formation of breast cancer.
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Keywords
Benign breast diseases, Malignant breast disease, Exonic splicing enhancers, Fhit gene, Novel mutations, Single-strand conformational polymorphism, Histidine triad gene, 3p14.2, Splicing enhancer motifs, Transcripts, Missense mutations, Brca1, Lung-cancer, Common, Expression, Lesions, Oncology
Citation
Çeçener, G. vd. (2007). "Importance of novel sequence alterations in the FHIT gene on formation of breast cancer". Tumori Journal, 39(5), 1662-1663.